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Trial registered on ANZCTR

Registration number

ACTRN12611000816954

Ethics application status

Approved

Date submitted

13/07/2011

Date registered

3/08/2011

Date last updated

29/08/2011

Type of registration

Prospectively registered

Titles & IDs

Public title

A randomised, open-label study to evaluate the efficacy and safety of maraviroc (MVC) as a switch for either nucleoside or nucleotide analogue reverse transcriptase inhibitors (N(t)RTI) or boosted protease inhibitors (PI/r) in HIV-1 infected individuals with stable, well-controlled plasma HIV-RNA while taking their first N(t)RTI + PI/r regimen of combination antiretroviral therapy (cART): MARCH study

Scientific title

Secondary ID [1]

KI-MARCH-01

Universal Trial Number (UTN)

Trial acronym

Linked study record

Health condition

Health condition(s) or problem(s) studied:

HIV

Condition category

Condition code

Inflammatory and Immune System

Other inflammatory or immune system disorders

Infection

Acquired immune deficiency syndrome (AIDS / HIV)

Intervention/exposure

Study type

Interventional

Description of intervention(s) / exposure

Maraviroc is a marketed drug for the treatment of HIV-infection. Maraviroc will be supplied in two different oral dose forms. 150mg and 300mg given twice a day. The drug will be dosed according to the recommendations in the product label i.e. with PI/r the dose is 150mg twice daily except, Miraviroc 300mg twice daily can be used at the discretion of the investigator if the PI/r is fosamprenavir/r, those randomised to the 2N(t)RTI arm, will recieve Maraviroc 300mg twice daily. Patients randomised to receive Miraviroc will be provided with bottles of Miravoroc at time points weeks 4, 12, 24, 36, 48, 60, 72, and 84. Each bottle contains a 30-day supply, however at the week 12 visit and ownards, the participant will receive 3 bottles.

There are 3 treatment arms in this study:
Arm 1 - No change i.e. continue their current cART regimen
Arm 2 - Replace N(t)RTI drugs with MVC at a dose of 150mg twice daily (MVC 300mg twice daily can be used at the discretion of the Investigator if the PI/r is fosamprenavir/r) and continue the PI/r
Arm 3 - Replace PI/r drugs with MVC at a dose of 300mg twice daily and continue 2N(t)RTI.

Treatment will continue until the last randomised participant has completed 96 weeks of follow-up or has permanently withdrawn from follow-up.

Intervention code [1]

Treatment: Drugs

Comparator / control treatment

No change: participants shall remain on their current cART regimen

Control group

Active

Outcomes

Primary outcome [1]

The comparison of the switch arms to control arm of proportions of participants with HIV RNA <200 copies/mL

Timepoint [1]

48 weeks after randomization

Secondary outcome [1]

Virologic endpoints
-Proportion of participants with plasma HIV-1 RNA <50 copies/mL
-Time to virological failure (defined as plasma HIV-1 RNA 200 copies/mL on randomised therapy, on two occasions at least seven days apart)
-Time to loss of virological response, as defined by virological failure, permanent randomised treatment discontinuation, new AIDS defining illness, death or withdrawal from study
-Changes from baseline in log plasma HIV-1 RNA copies/mL
-Frequency of plasma HIV-1 RNA blips (defined as a plasma viral load result >200 copies/mL on randomised therapy following a previous result <200 copies/mL, with a follow up result <200 copies/mL at least seven days after the >200 copies/mL reading, in the absence of a change of any component of the ART regimen).

Timepoint [1]

48 weeks after randomization

Secondary outcome [2]

Immunologic and biomarker endpoints
-Changes from baseline in absolute and percentage CD4+ and CD8+T cells
-Changes from baseline in selected soluble markers of immune activation/coagulation.

Timepoint [2]

48 weeks after randomization

Secondary outcome [3]

Clinical endpoints
-Rate of opportunistic disease (AIDS) or death
-Rates of serious non AIDS defining illness and non AIDS related mortality.

Timepoint [3]

48 weeks after randomization

Secondary outcome [4]

Metabolic and body composition endpoints
-Changes from baseline in fasting lipids (TC, LDL, HDL and TG)
-Changes in absolute CVD risk assessment using the Framingham risk equation
-Changes from baseline in fasting glucose and insulin
-Rates of initiation or changes in existing lipid lowering therapies
-Changes from baseline in anthropometric changes derived from Dual energy X ray absorptiometry (DXA) scanning of peripheral and central adipose tissue
-Changes from baseline in bone mineral density and body fat as measured by DXA
-Changes in 10 year fracture risk using the FRAX algorithm
-Changes from baseline in markers of bone turnover.

Timepoint [4]

48 weeks after randomization

Secondary outcome [5]

Safety
-Changes from baseline in selected serum biochemical parameters, including changes in estimated glomerular filtration rate (GFR)

Timepoint [5]

48 weeks after randomization

Secondary outcome [6]

Adherence
-Self reported adherence to randomised study medications.

Timepoint [6]

48 weeks after randomization

Secondary outcome [7]

Quality of Life
Change from baseline health status scores as measured by the SF12 questionnaire.

Timepoint [7]

48 weeks after randomization

Secondary outcome [8]

Resistance endpoints
-Patterns of genotypic resistance at virological failure.

Timepoint [8]

48 weeks after randomization

Eligibility

Key inclusion criteria

1. Documented HIV-1 infection by a licensed diagnostic test at any time prior to study entry
2. Age >18 years
3. HIV-1 RNA <200 copies/mL plasma for at least 24 weeks
4. Stable (>24 weeks) ART including two N(t)RTIs and a PI/r
5. No evidence of any primary HIV genotypic mutations in HIV reverse transcriptase or protease for all patients with available resistance testing results conducted prior to cART and/or during viral rebound/failure
6. Provision of written, informed consent.

Minimum age

18 Years

Maximum age

No limit

Sex

Both males and females

Can healthy volunteers participate?

Key exclusion criteria

1. CXCR4 or CCR5/CXCR4 dual tropic HIV tropism or a non-reportable tropism result based on assessment using proviral DNA
2. Anticipated need to modify current cART regimen for toxicity management in the next 6 months
3. The following laboratory criteria,
a. absolute neutrophil count (ANC) <750 cells/micro L
b. haemoglobin <8.0 g/dL
c. platelet count <50,000 cells/micro L
d. serum AST, ALT >5 x upper limit of normal (ULN)
4. Active hepatitis B co-infection
5. Pregnant women or nursing mothers
6. Current use of any prohibited medications as described in product specific information.
7. Hypersensitivity to soy or peanuts
8. Acute therapy for serious infection or other serious medical illness (in the judgement of the site Principal Investigator) requiring systemic treatment and/or hospitalisation
9. Use of immunomodulators (e.g. systemic corticosteroids, recombinant interleukin-2, interferon) within 30 days prior to screening
10. Patients with current alcohol or illicit substance use that in the opinion of the site Principal Investigator would conflict with any aspect of the conduct of the study
11. Patients unlikely to be able to remain in follow-up for the protocol-defined period
12. Prisoners or subjects who are compulsorily detained (involuntary incarcerated).

Study design

Purpose of the study

Treatment

Allocation to intervention

Randomised controlled trial

Procedure for enrolling a subject and allocating the treatment (allocation concealment procedures)

Methods used to generate the sequence in which subjects will be randomised (sequence generation)

Masking / blinding

Open (masking not used)

Who is / are masked / blinded?

Intervention assignment

Parallel

Other design features

Phase

Phase 4

Type of endpoint/s

Safety/efficacy

Statistical methods / analysis

Recruitment

Recruitment status

Recruiting

Date of first participant enrolment

Anticipated

26/08/2011

Actual

Date of last participant enrolment

Anticipated

Actual

Date of last data collection

Anticipated

Actual

Sample size

Target

560

Accrual to date

Final

Recruitment in Australia

Recruitment state(s)

Recruitment outside Australia

Country [1]

Argentina

State/province [1]

Country [2]

Canada

State/province [2]

Country [3]

Chile

State/province [3]

Country [4]

Germany

State/province [4]

Country [5]

Ireland

State/province [5]

Country [6]

Israel

State/province [6]

Country [7]

Mexico

State/province [7]

Country [8]

Peru

State/province [8]

Country [9]

Spain

State/province [9]

Country [10]

United Kingdom

State/province [10]

Country [11]

France

State/province [11]

Country [12]

Japan

State/province [12]

Funding & Sponsors

Funding source category [1]

Commercial sector/Industry

Name [1]

Pfizer Inc., a Delaware Corporation

Address [1]

235 East 42nd Street
New York
New York 10017

Country [1]

United States of America

Primary sponsor type

University

Name

University of New South Wales, Kirby Institute

Address

Cliffbrook Campus
45 Beach Street
Coogee
New South Wales 2034

Country

Australia

Secondary sponsor category [1]

None

Name [1]

Address [1]

Country [1]

Ethics approval

Ethics application status

Approved

Ethics committee name [1]

St. Vincent's Hospital Human Research Ethics Committee

Ethics committee address [1]

Level 6, De Lacy Building
St. Vincent's Hospital
390 Victoria Street
Darlinghurst
New South Wales 2010

Ethics committee country [1]

Australia

Date submitted for ethics approval [1]

23/05/2011

Approval date [1]

Ethics approval number [1]

11/065

Summary

Brief summary

MARCH is an international, multicentre trial planning to enroll 560 HIV-1 infected patients who are currently on 2N(t)RTI + PI/r regimen and virologically suppressed. Participants will be randomized (1:2:2) to one of three treatment groups: to continue their current treatment regimen, maraviroc dose at 150 mg twice daily with PI/r, or maraviroc at 300 mg twice daily with 2N(t)RTI. As the participants population have HIV RNA <200 copies/mL, the phenotypic assessment of tropism cannot be used to determine tropism, instead we will employ the genotypic assessment of tropism by sequencing the V3 loop of the HIV envelope. The main aim of this study is to investigate whether switching to maraviroc, in combination with either RTI or PI/r, is as good at keeping the HIV viral load undetectable as the combination of RTI with PI/r.  The other aim is to see if switching to these combinations with maraviroc will improve some of the side effects that can be seen when people take combination therapy including RTI and PI/r.
The study hypothesis is that in stable, virologically suppressed (plasma HIV-RNA <200 copies/mL) patients with no history of prior virological failure, a switch to either MVC dosed at 300mg twice daily (bid) combined with the same 2N(t)RTI backbone regimen or MVC dosed at 150mg twice daily (bid) with the current PI/r (or 300mg bid at the discretion of the investigator if the PI/r is fosamprenavir/r) provides similar (non-inferior) antiretroviral efficacy compared to continuation of the current 2N(t)RTI + PI/r regimen.

Trial website

Kirby Institute for infection and immunity in society homepage - click here for more information on the MARCH study:  
          http://www.kirby.unsw.edu.au

Trial related presentations / publications

Public notes

Contacts

Principal investigator

Name

Address

Country

Phone

Fax

Contact person for public queries

Name

Dr Sarah L. Pett

Address

Kirby Institute, Faculty of Medicine, UNSW
Cliffbrook Campus, Building CC4, Level 2
45 Beach Street
Coogee
NSW 2034

Country

Australia

Phone

+61-2-9385-0900

Fax

+61.2.9385.0910

[email protected]

Contact person for scientific queries

Name

Prof. David A. Cooper

Address

Kirby Institute, Faculty of Medicine, UNSW
Cliffbrook Campus, Building CC4, Level 2
45 Beach Street
Coogee
NSW 2034

Country

Australia

Phone

+61.2.8382.4904

Fax

+61.2.9385.0910

[email protected]

No information has been provided regarding IPD availability

What supporting documents are/will be available?

No Supporting Document Provided

Results publications and other study-related documents

Documents added manually

No documents have been uploaded by study researchers.

Documents added automatically

No additional documents have been identified.

Trial Review

Documents added manually

Documents added automatically